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Studies Explore Roles of Chemotherapy and Radiotherapy in Hodgkin’s Disease

Studies Explore Roles of Chemotherapy and Radiotherapy in Hodgkin’s Disease

February 01, 1999

MIAMI BEACHHodgkins disease (HD) was the focus of
an education session and major new research reports at the American
Society of Hematology annual meeting. Among the conclusions:
Neoadjuvant chemotherapy before radiotherapy provides better outcomes
in early-stage HD; moderate dose escalation offers some advantages in
advanced disease; and chemotherapy is equal to radiotherapy as
consolidation treatment in advanced disease.

Neoadjuvant Chemotherapy

An interim analysis from the German Hodgkins Lymphoma Study
Group HD7 trial found that two cycles of ABVD plus radiotherapy is
more effective than radiotherapy alone in early-stage HD. Two
cycles of ABVD prior to extended-field radiotherapy reduces the
relapse rate and improves the time to treatment failure, Hans
Tesch, MD, of the University of Cologne, reported for the investigators.

Dr. Tesch said that extended-field radiotherapy produces complete
remissions in more than 90% of patients with early-stage HD, but that
up to 25% eventually relapse and require intensive chemotherapy. This
trial was undertaken to determine whether low-dose neoadjuvant
chemotherapy could reduce the risk of relapse.

The trial included 640 patients with stage I or II Hodgkins
disease who did not have poor prognostic factors (large mediastinal
mass, massive spleen involvement, extranodal disease, elevated ESR,
more than 3 lymph node areas).

Patients were randomized to receive either extended-field
radiotherapy with 30 Gy, plus involved-field radiation of 40 Gy and
spleen radiation of 36 Gy, or two cycles of ABVD (doxorubicin,
bleomycin, vindesine, dacarbazine) followed by the same radiotherapy schedule.

The median follow-up of this interim analysis was 28 months and
included 365 patients. The complete response rate was 96% with
radiotherapy alone and 98% with ABVD plus radiotherapy.

Kaplan-Meier estimates of freedom from treatment failure showed a
significant difference in favor of ABVD plus radiotherapy (87% vs 96%
at 24 months, P < .05). The difference is due mainly to the
reduction in the number of relapses with combination therapy (9% vs
1%). Survival rates are not different at 24 months (97% vs 98%).
There were seven deaths in each treatment arm.

Acute toxicities were rare on both treatment arms, but Dr. Tesch said
that 11% of patients on the ABVD/radiotherapy arm developed leukopenias.

Dr. Tesch concluded, The interim analysis demonstrates that
neoadjuvant chemotherapy with two cycles of ABVD significantly
reduces the rate of relapse and improves the time to treatment
failure. Current trials with combined modality therapy aim to reduce
acute and long-term toxicities by reducing radiotherapy dose and volume.

Moderate Dose Escalation

At least 40% of patients with advanced stage HD will eventually have
disease recurrence or progression. Volker Diehl, MD, reporting a
second interim analysis for the German Hodgkins Lymphoma Study
Group HD9 trial, said that moderate chemotherapy dose escalation
improves time to progression in advanced-stage Hodgkins disease.

Baseline BEACOPP was approximately equivalent in dosage to COPP/ABVD
but shortened to a 3-week course. On the escalated arm, compared with standard
BEACOPP, doses were escalated to 192% cyclophosphamide, 200%
etoposide, and 140% doxorubicin.

Dr. Diehl said that etoposide, doxorubicin, and cyclophosphamide were
given on days 1 to 3 and repeated on day 21 in order not to
give the cells time to develop resistance. The standard
COPP/AVBD arm was stopped early on in the study.

The study enrolled 1,055 patients between 15 and 65 years of age with
either stage IIB/IIIA disease with risk factors or stage
IIIB/IV disease. Eight courses of chemotherapy were followed by local
irradiation of initial bulky and residual disease. Median observation
time was 27 months.

Acute toxicity (neutropenia, thrombocytopenia, anemia, infection)
under BEACOPP was increased but manageable; toxic deaths
were not more frequent than for COPP/ABVD. Progressive HD accounted
for 11 of 29 deaths on standard therapy, 9 of 17 deaths on BEACOPP,
and 1 of 9 deaths on escalated BEACOPP.

Another approach in advanced-stage Hodgkins disease is to use
radiotherapy rather than chemotherapy as consolidation therapy.

Christophe Fermé, MD, reporting for the Groupe dEtude
des Lymphomes de lAdulte (GELA), Hôpital Saint-Louis,
Paris, France, said that these two approaches produced essentially
the same results in stage IIIB-IV Hodgkins disease in first
complete remission or good partial response. There were no
significant differences in either overall survival or 5-year event-free
survival in this study.

The 559 patients in this study were randomized at diagnosis to
receive six cycles of ABVPP (doxorubicin, bleomycin, vinblastine,
procarbazine, prednisone) or MOPP/ABV hybrid.

Patients in complete response or 75% partial response after six
cycles were then randomized to receive either two additional cycles
of the same regimen or radiotherapy. This included subtotal or total
nodal irradiation of 30 Gy, plus 5 Gy to the initially involved areas
and 5 Gy to the residual mass.

Dr. Fermé said that at a median follow-up of 46 months, 152
patients (28%) had progressed and 90 had died, 43 of HD and 47 of
other causes, including seven solid tumors, five non-Hodgkins
lymphomas, and one AML. Three other patients developed secondary AML
and are alive without Hodgkins disease.

He concluded that chemotherapy alone allows the same survival
or a better survival than chemotherapy plus radiotherapy but
that a longer follow-up, analysis of fatal events, and analysis of
salvage from relapse after radiotherapy will be required to give
definitive conclusions about these two approaches to consolidation.

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